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Independent molecular development of metachronous glioblastomas with extended intervening recurrence-free interval.

机译:异时性胶质母细胞瘤的独立分子发展,介入无复发间隔延长。

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摘要

Two metachronous glioblastomas with different cerebral locations in a 53-year-old long-term survival patient were analyzed by multiple genetic approaches. Using comparative genomic hybridization a different pattern of chromosomal aberrations was observed, with 19 imbalances in the first tumor and only 2 imbalances in the second. Sequence analysis revealed a distinct mutation profile in each tumor, with amino acid substitutions in the p53 and PTEN genes only in the first tumor, ie, p53 in codon 273 (CGT-->TGT, Arg-->Cys) and PTEN in codon 336 (TAC-->TTC, Tyr-->Phe). A splicing acceptor site PTEN mutation (IVS8-2A>G) was observed only in the second GBM. EGFR amplification, mutations of p16INK4a/CDKN2A or p14ARF were not observed. According to the results of p53 mutational analysis and EGFR amplification studies, the first tumor is classified as a type 1 GBM, whereas the alterations in the second one are different from those typically encountered in type 1 or type 2 tumors. In conclusion, our data strongly suggest that the metachronous tumors in this patient are exceptional in that they developed independently from each other. Whether the molecular features of the first glioblastoma are associated with the notably extended recurrence-free period of 5 years remains to be elucidated.
机译:通过多种遗传学方法分析了53岁的长期存活患者中两个大脑位置不同的异时性胶质母细胞瘤。使用比较基因组杂交,观察到不同的染色体畸变模式,第一个肿瘤中有19个失衡,第二个肿瘤中只有2个失衡。序列分析揭示了每个肿瘤中独特的突变谱,仅在第一个肿瘤中p53和PTEN基因被氨基酸取代,即密码子273(CGT-> TGT,Arg-> Cys)中的p53和密码子中的PTEN 336(TAC-> TTC,Tyr-> Phe)。仅在第二GBM中观察到剪接受体位点PTEN突变(IVS8-2A> G)。未观察到EGFR扩增,p16INK4a / CDKN2A或p14ARF突变。根据p53突变分析和EGFR扩增研究的结果,第一个肿瘤被分类为1型GBM,而第二个肿瘤的变化与1型或2型肿瘤通常遇到的变化不同。总之,我们的数据有力地表明,该患者的异时性肿瘤是例外的,因为它们彼此独立发展。第一个胶质母细胞瘤的分子特征是否与5年显着延长的无复发期有关还有待阐明。

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